Target Modulation by a Kinase Inhibitor Engineered to Induce a Tandem Blockade of the Epidermal Growth Factor Receptor (EGFR) and c-Src: The Concept of Type III Combi-Targeting

Rao, Suman; Larroque-Lombard, Anne-Laure; Peyrard, Lisa; Thauvin, Cédric; Rachid, Zakaria; Williams, Christopher; Jean‐Claude, Bertrand J.

doi:10.1371/journal.pone.0117215

Cited by 25 publications

(25 citation statements)

References 49 publications

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“…With the EGFR-expressing 4T1 tumor model (26), we stratified excised tumors into “low,” “medium,” and “high” antibody groups. Co-injected TNP-encapsulated docetaxel was then quantified.…”

Section: Resultsmentioning

confidence: 99%

Predicting therapeutic nanomedicine efficacy using a companion magnetic resonance imaging nanoparticle

et al. 2015

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Therapeutic nanoparticles (TNPs) have shown heterogeneous responses in human clinical trials, raising the question of whether imaging should be used to identify patients with a higher likelihood of nanoparticle accumulation, and thus therapeutic response. Despite extensive debate about the enhanced permeability and retention (EPR) effect in tumors, it is increasingly clear that EPR is extremely variable yet little experimental data exists to predict its clinical utility. Based on the hypothesis that an FDA-approved 30-nm magnetic nanoparticle (MNP) could predict co-localization of therapeutic nanoparticles by MRI, we performed single-cell resolution imaging of fluorescently labeled MNPs and TNPs and studied their intratumoral distribution. We visualized MNPs circulating in tumor microvasculature and found sustained uptake into cells of the tumor microenvironment within minutes. MNPs could predictably demonstrate areas of co-localization for a model TNP [poly(D,L-lactic-co-glycolic acid)-b-polyethylene glycol; PLGA-b-PEG] within the tumor microenvironment (> 85% accuracy) and circulating within the microvasculature (>95% accuracy) despite their markedly different sizes and compositions. Computational analysis of NP transport enabled predictive modeling of TNP distribution based on imaging data, and identified key parameters governing intratumoral NP accumulation and macrophage uptake. Finally, MRI imaging accurately predicted initial treatment response and drug accumulation in a therapeutic study testing for the efficacy of paclitaxel-encapsulated nanoparticle. These approaches yield valuable insight into the in vivo kinetics of NP distribution and suggest that clinically-relevant imaging can be used to select patients with high EPR for treatment with TNPs.

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Section: Resultsmentioning

confidence: 99%

Predicting therapeutic nanomedicine efficacy using a companion magnetic resonance imaging nanoparticle

et al. 2015

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“… 1 c-Src, a prometastasis oncogene, is well characterized to promote cellular invasion, migration and has been justly proposed as a therapeutic target in cancers. 2 , 3 , 4 , 5 However, the biochemical regulation of c-Src activation is not fully understood. The best-characterized Src regulator is phosphorylation, with the two major sites of phosphorylation on murine and chicken c-Src being Tyr416 (Tyr419 in humans) and Tyr527 (Tyr530 in humans).…”

Section: Introductionmentioning

confidence: 99%

Dual-faced SH3BGRL: oncogenic in mice, tumor suppressive in humans

et al. 2015

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Despite abundant data supporting c-Src as a metastasis-promoting oncogene, activating mutations of c-Src are rare. This suggests that trans-interacting proteins may have a critical role in regulating c-Src activation. Here, we first report the discovery of Src homology 3 (SH3) domain-binding glutamic acid-rich-like protein (SH3BGRL), a novel c-Src activator in mice. Ectopic expression of murine SH3BGRL (mSH3BGRL) strongly promoted both tumor cell invasion and lung metastasis. Molecularly, mSH3BGRL specifically bound the inactive form of c-Src phosphorylated at Tyr527, promoting Tyr416 phosphorylation of c-Src and subsequent FAK-mediated activation of ERK and AKT signaling pathways. Targeting endogenous c-Src alone was sufficient to abolish mSH3BGRL-induced cancer metastasis in vivo. Unexpectedly, human SH3BGRL (hSH3BGRL) in turn suppressed tumorigenesis and metastasis in nature. We attempted site-specific reversion of hSH3BGRL amino-acid sequence to mSH3BGRL and found V108A substitution sufficient to restore SH3BGRL function as a c-Src activator and metastasis promoter. Notably, the somatic mutation R76C of hSH3BGRL can similarly act as hSH3BGRL-V108A and mSH3BGRL in tumorigenesis and metastasis. Our results uncover an evolutionarily controversial role of SH3BGRL in driving tumor metastasis through c-Src activation, and suggests that hSH3BGRL mutation status could be relevant to cancer diagnosis and therapy.

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“…It has previously been shown that ROCK inhibition by Y-27632 can inhibit the infiltration of MDA-MB-231 cells using 2D in vitro assays 102 – 104 . Conversely, the EGFR inhibitor Gefitinib has been shown to have potent anti-proliferative effects on MDA-MB-231 cells 105 – 107 , while the anti-invasive effect is less well established 108 – 110 . To quantify the changes in invasion depth upon inhibition, invaded MDA-MB-231 cells at each 100 μm increment were divided by the number of cells on the surface of the collagen matrix, in a similar manner to the invasive index calculated in Fig.…”

Section: Resultsmentioning

confidence: 99%

Three-dimensional organotypic matrices from alternative collagen sources as pre-clinical models for cell biology

Conway

Vennin

Cazet

et al. 2017

Sci Rep

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Organotypic co-cultures bridge the gap between standard two-dimensional culture and mouse models. Such assays increase the fidelity of pre-clinical studies, to better inform lead compound development and address the increasing attrition rates of lead compounds within the pharmaceutical industry, which are often a result of screening in less faithful two-dimensional models. Using large-scale acid-extraction techniques, we demonstrate a step-by-step process to isolate collagen I from commercially available animal byproducts. Using the well-established rat tail tendon collagen as a benchmark, we apply our novel kangaroo tail tendon collagen as an alternative collagen source for our screening-ready three-dimensional organotypic co-culture platform. Both collagen sources showed equal applicability for invasive, proliferative or survival assessment of well-established cancer models and clinically relevant patient-derived cancer cell lines. Additional readouts were also demonstrated when comparing these alternative collagen sources for stromal contributions to stiffness, organization and ultrastructure via atomic force microscopy, second harmonic generation imaging and scanning electron microscopy, among other vital biological readouts, where only minor differences were found between the preparations. Organotypic co-cultures represent an easy, affordable and scalable model to investigate drug responses within a physiologically relevant 3D platform.

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Target Modulation by a Kinase Inhibitor Engineered to Induce a Tandem Blockade of the Epidermal Growth Factor Receptor (EGFR) and c-Src: The Concept of Type III Combi-Targeting

Cited by 25 publications

References 49 publications

Predicting therapeutic nanomedicine efficacy using a companion magnetic resonance imaging nanoparticle

Predicting therapeutic nanomedicine efficacy using a companion magnetic resonance imaging nanoparticle

Dual-faced SH3BGRL: oncogenic in mice, tumor suppressive in humans

Three-dimensional organotypic matrices from alternative collagen sources as pre-clinical models for cell biology

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